Zakia M, Shalabi T, Hussein T, Hammam M, Youness E, El-Bassyouni H. T. Oxidative Stress, Neutrophil Elastaseand Vascular Endothelial Growth Factor in Obese Pregnant Women with Preeclampsia. Biomed Pharmacol J 2019;12(4).
Manuscript received on :03-09-2019
Manuscript accepted on :05-11-2019
Published online on: 07-12-2019
Plagiarism Check: Yes
Reviewed by: Hendry Irawan
Second Review by: Pietro Scicchitano
Final Approval by: Dr Ayush Dogra

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Moushira Zakia1, Taghreed Shalabi2, Tamer Hussein3, Mohamed Hammam4, Eman Youness5* and Hala T. El-Bassyouni6

Corresponding Author Email: hoctober2000@yahoo.com

1Biological Anthropology Department, Medical Research Division, National Research Centre,Egypt

2Prenatal Diagnosis and Fetal Medicine Department, Human Genetics and Genome Research Division, National Research Centre, Egypt

3Reproductive Health Research Department, Medical Research Division, National Research Centre, Egypt

4Obstetrics and Gynecology-Cairo University

5Medical Biochemistry Department, Medical Research Division, National Research Centre, Egypt

6Clinical Genetics Department,Human Genetics and Genome Research Division, National Research Centre, Giza, Egypt

DOI : https://dx.doi.org/10.13005/bpj/1819

Abstract

Oxidative stress, inflammation, and vascular endothelial proliferation and obesity are risk factors associated with preeclampsia (PE). Thepresent study aimed to investigate the levels of malondialdehyde (MDA) as a putative circulatory marker of oxidative stress, neutrophil Elastase (NE) as inflammatory marker andvascular endothelial growth factor (VEGF) as marker for vascular permeability-enhancing activities inobese women withpreeclampsia PE and compare withnormal pregnancy women. The study was carried out on 50 pregnant obese women with PE and 50 normal pregnant women.  The preeclampsia women were characterized with high blood pressure 160/110 mmHg and proteinuria. The gestational age ranged from ≥32 weeks to <37 weeks. Pre pregnancyweightwas recorded. Body mass index (BMI) was calculatedat delivery.SerumMDA, NEand VEGF were estimatedby ELISA. Significant higher levels of serum MAD,NE and VEGF were observed in obese PE patients as compared to normal controls. Our results suggested thatobesity;oxidative stress, NEandVEGFbiomarkers are risk factors for PE,emphasizing their role as feasible candidate risk markersfor cases withhigh blood pressure in early pregnancy.

Keywords

Malonaldehyde; Neutrophil Elastase; Preeclampsia; VEGF

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Zakia M, Shalabi T, Hussein T, Hammam M, Youness E, El-Bassyouni H. T. Oxidative Stress, Neutrophil Elastaseand Vascular Endothelial Growth Factor in Obese Pregnant Women with Preeclampsia. Biomed Pharmacol J 2019;12(4).

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Zakia M, Shalabi T, Hussein T, Hammam M, Youness E, El-Bassyouni H.T. Oxidative Stress, Neutrophil Elastaseand Vascular Endothelial Growth Factor in Obese Pregnant Women with Preeclampsia. Biomed Pharmacol J 2019;12(4). Available from: https://bit.ly/38fjaKF

Introduction

Hypertension and proteinuria are pregnancy-specific conditions characterize dpreeclampsia. Although its precise etiology is unknown,endothelial cell dysfunction might causematernal symptoms1.The major cause of maternal and perinatal morbidity and mortality is preeclampsia, 10%of women had high blood pressure during pregnancy2.

Moreover,preeclampsiamight lead to problems in the kidneys, liver, clotting system and brain in 2% to 8% of pregnancies, with premature andpoor and growth offspring.Although outcome is often good, preeclampsia can be harmful and life threatening.

Generally, preeclampsia and eclampsia are concomitant with direct maternal deaths  in 10% to 15% 3. The pathophysiology of preeclampsia has been implicated byneutrophils activation whichengaged binding and transmigration of neutrophils through the endothelium4 , through surface receptors on neutrophils and endothelium adhesion molecules.women with preeclampsia showed stimulated neutrophils which plays an important role in the vascular endothelium pathophysiology of this disorder5.Amplified numbers of neutrophils are notedfrom first to third trimesterin the maternal circulation, with elevated neutrophil count. Consequently,unfavorable pregnancy outcome might linked to excessive inflammatory neutrophil activation andincreased concentration of elastase discharged from neutrophil granules 6.Oxidative stress and oxidative damage in early gestation in early gestation influences the onset of these conditions later in pregnancy7,8.  Increased oxidative stress markers perform significant role in the pathophysiology of preeclampsia<sup>9</sup>9,10. Increase in the free radicalscauses overproduction of MDA which is the indicator of oxidativestress6,7.

An important angiogenic factor was described to provoke the proliferation and migration of endothelial cells is vascular endothelial growth factor (VEGF), enhances vascular permeability, and modulates thrombogenicity. Consequently, it is implicated indevelopment of normal bloodvessel as well as in vascular pathologies11.

The present study aimed to evaluate and compare the biomarker variables of oxidative stress, inflammatory and cytokine VEGF in preeclamptic women andin normal pregnant women.

Material and Methods

The blood samples were collected from 50 preeclamptic and 50 normal pregnant women at the department of obstetrics and gynecology, Cairo University and National Research Centre. The study was approved by the Ethical Committee form of National Research Centre, Egypt (number = 16361), in accordance with the World Medical Association’s Declaration of Helsinki.The age of the women ranged from 25-40 years, their mean age was 34.31 ± 8.83 andpre pregnancy BMI (kg/m2) was29.9 ± 6.91.

Circulating markers of oxidative stress MDA, neutrophil elastase and vascular endothelial growth factor (VEGF)were evaluatedamong women with and without preeclampsia.

A dipstick urine measurement for protein was performed on urine specimen collected from the patient on the clinic days. Testing was performed with multistix reagent strips (Bayer). Proteinuria was classified semi-quantitatively as absent if testing with a dipstick showed no protein or trace levels (level below 300 mg L-1); low grade if the dipstick showed a value of 1+ or 2+(level between 300 and 3000 mg L-1) and high grade if the dipstick showed a value of 3+ or 4+(level>3000 mg L-1).Proteinuria was observed with low grade in 46 % and with high grade in 54% of cases.

Statistical analyses

Statistical analyses were performed with SPSS software, version 19.0 (SPSS Inc., Chicago, IL, USA)taking level of significance to be p<0.05.Normal distributionof the data for each parameter was checked by Kolmogorov-Smirnov analysis. Percentage, mean, and standard deviationwere used to express normally distributed variables. An unpaired t-test was applied to determine the mean significant difference between normal and preeclamptic groups. Percentage distribution in preeclampsia women was done by using chi-square test.

Results

A total of 100 women were enrolled, 50 obese women with preeclampsia and 50 normotensive controls.The obstetric history shows that the mean gestational age at delivery was 33.54±5.68 in PE. The mean number of pregnancies was 3.69 ±1.932.The systolic blood pressures was 172.69 ± 12.85, diastolic blood pressure was 111.92 ± 9.02. PE showed significant higher BMI 32.94 ± 8.93 than normal controls. Moreover, the pre-pregnancy BMI was significantly higher in PE women. Proteinuria was observed in PE with low grade in 46 % and with high grade in 54 % and deliveries withprevious miscarriages was 92% in PE and 2% in normal controls(table 1).Statistically significant difference was observed between PE and controls in the mean levels of blood pressure and in frequency of previous miscarriages (p <0.05). Moreover, MDA levels were significantly higher among the preeclampsia patients (5.23 ± 2.58) as comparedto normal control group (0.91 ± 0.29)as well as NE in the preeclampsia patients(7.52 ± 2.60) compared tonormal control group (3.45 ± 1.23) and VEGF(122.68 ± 16.69) in PE compared to normal pregnancy(82.68 ± 10.14)(table 2) (P < 0.05).

Table 1: Clinical characteristic ofnormal controls and women with preeclampsia

Normal Control Pregnancies

Mean ± SD

Preeclampsia

Mean ± SD

Maternal age (years) 36.31 ± 8.835 34.31 ± 8.835
Pre-pregnancy BMI(kg/m2) 22.9 ± 4.93 30.9 ± 6.91*
Gestational age at delivery (weeks) 35.54 ± 2.61 33.54 ± 5.68
Number of pregnancies 3.69 ±1.932 3.69 ±1.932
Systolic blood pressure (mmHg)

 

114.9 ± 6.7 172.69 ± 12.84*
Diastolic blood pressure(mmHg) 73.67± 5.5 111.92 ± 9.02*
Body Mass Index (kg/m2) 23.22 ± 6.91 32.94 ± 8.93*
Deliveries with previous miscarriages [n (%)] 

 

1(2%) 46 (92%)*
Cases presenting with proteinuria 1+ or 2+[n (%)]  23(46%)
Cases presenting with proteinuria 3+ or 4+[n (%)]  27 (54%)

* P ≤ 0.05: PE vs. healthy pregnant women

Table 2: Thelevels of malonaldehyde, neutrophil elastaseandVEGF in preeclampsia

Malonaldehyde

(µmole/L)

Neutrophil elastase

(µmole/L)

VEGF

(pg/ml)

Women with preeclampsia 5.23 ± 2.58* 7. 52 ± 2.60*

 

122.68 ± 16.69*
Normal Control Pregnancies

 

0.91 ± 0.29 3.45 ± 1.23 82.68 ± 10.14

* P ≤ 0.05: PE vs. healthy pregnant women

Discussion

PE is clinically detected after 20 weeks’ gestationand potentially life-threatening. It affects 5% of pregnancies and is characterized by hypertension and proteinuria in mild cases, and evenseizures, organ damage and maternal death in severe cases. In our study we found that the mean age was 34.31±8.835, not all of our cases were primigravida with the mean number of pregnancies 3.69±1.932.Similarly,  other study 12 described preeclamptic women with maternal age31.0 ± 4.6. This report stated that the gestational age in their patients was 33.54±5.68 and the mean BMI was 32.94±8.93 this coincides with the findings of Sharma et al., 2006 and Wang et al., 2017who reported preeclamptic women with gestational age35.2 ± 3.6 and BMI 25.86 ± 2.82.Moreover,Sohlberg et al., 2012 elucidated that the high maternal body mass index increases the risk of preeclampsia. Likewise, inprevious studies done on extremely obese teenagers they detected that they were almost four times likely to develop preeclampsia and eclampsia compared with non-obese women. However, obesity elevated the risk for preeclampsia and eclampsia among all women in the study, teenagers were most at risk because of the compound effect of young age and obesity8,9.

Magee et al., 2014 reported that ISSHP-definitionof pre-eclampsia occur whenthe systolic blood pressure is > 140 mmHg and diastolic blood pressure is > 90 mmHgdevelopingafter 20 weeksgestational age.

In our study the mean systolic blood pressure was 172.69±12.84 and the mean diastolic blood pressure 111.92±9.02 in women with preeclampsia which is higher than thenormal control pregnancy.Proteinuria (> 300 mg/day) occurs in preeclampsia and classified as low grade +1 or +2 which occurred in 46% of our cases and moderate and high grade in 54% of cases.

In PE, OS induced in the ischemic placenta producesthe release of cytotoxic factors into the maternal circulation, stimulating the inflammatory response and activating maternal endothelial cells 6,15.During normal pregnancy, placental oxidative stress (OS) is present during all three trimestersand is necessary to obtain normal cell function. However, if OS reaches a certain level, pregnancy complications might develop3,15. PE is related to an impaired endothelial function that accounts foractivation of the coagulation cascade,altered vascular reactivity and loss of vascular integrity. Impaired endothelial malondialdehyde levels were significantly higher as shown in the study done by 16,17. Preeclampsia is a chronic inflammatory disease in pregnancy, which is associated with damaged maternal endothelium a potent stimulator for neutrophil activation18. Neutrophils are increased due to augmentedphysiologic stress and impaired neutrophilic apoptosis during pregnancy19. Elevated levels of VEGF in preeclamptic women compared to normal pregnant was reported in some studies11,20. However, other studies delineated decreased level of serum VEGF in preeclamptic women 21.  The decrease in VEGF level becomes more significant with increasing PE severity, proposing that the decrease in VEGF synthesis and release may be an important factor in PEpathogenesis 22. The association between of preeclampsia and high BMI reported in our study is consistent with other studies23,24.Pre-pregnancy obesity was observed in our study in agreement with previous studies reported association between re-pregnancy BMI and preeclampsia25,26

Conclusion: Combination of obesity, elevated MDA, NE and VEGF biomarkers in the early third trimester may be important risk factors in PE pathogenesis and could predict cases at risk of high-normal blood pressure in early pregnancy.

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